US12241950B2 - Magnetoresistive sensor array for molecule detection and related detection schemes - Google Patents
Magnetoresistive sensor array for molecule detection and related detection schemes Download PDFInfo
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- C12Q2565/00—Nucleic acid analysis characterised by mode or means of detection
- C12Q2565/60—Detection means characterised by use of a special device
- C12Q2565/629—Detection means characterised by use of a special device being a microfluidic device
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- G11B5/02—Recording, reproducing, or erasing methods; Read, write or erase circuits therefor
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- G11B5/127—Structure or manufacture of heads, e.g. inductive
- G11B5/33—Structure or manufacture of flux-sensitive heads, i.e. for reproduction only; Combination of such heads with means for recording or erasing only
- G11B5/39—Structure or manufacture of flux-sensitive heads, i.e. for reproduction only; Combination of such heads with means for recording or erasing only using magneto-resistive devices or effects
- G11B5/3903—Structure or manufacture of flux-sensitive heads, i.e. for reproduction only; Combination of such heads with means for recording or erasing only using magneto-resistive devices or effects using magnetic thin film layers or their effects, the films being part of integrated structures
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- G11B5/33—Structure or manufacture of flux-sensitive heads, i.e. for reproduction only; Combination of such heads with means for recording or erasing only
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- G11B5/3903—Structure or manufacture of flux-sensitive heads, i.e. for reproduction only; Combination of such heads with means for recording or erasing only using magneto-resistive devices or effects using magnetic thin film layers or their effects, the films being part of integrated structures
- G11B5/3906—Details related to the use of magnetic thin film layers or to their effects
- G11B5/3909—Arrangements using a magnetic tunnel junction
Definitions
- Embodiments of the present disclosure generally relate to magnetoresistive (MR) sensor arrays for detection of molecules coupled to magnetic nanoparticles (MNPs), such as for nucleic acid sequencing such as deoxyribonucleic acid (DNA) sequencing, and methods of using such MR sensor arrays for molecule detection.
- MNPs magnetoresistive
- DNA deoxyribonucleic acid
- the Rayleigh criterion currently represents the fundamental limitation for inward scaling of optical SBS systems which can only be overcome by applying super-resolution imaging techniques (see A. M. Sydor, K. J. Czymmek, E. M. Puchner, and V. Mannella, “Super-Resolution Microscopy: From Single Molecules to Supramolecular Assemblies”, Special Issue: Quantitative Cell Biology, Vol. 25, 730, 2015) and has not yet been achieved in highly multiplexed systems.
- increasing throughput and decreasing cost of optical SBS sequencers has been slow due to the need to build bigger flow cells and implement more expensive optical scanning and imaging systems.
- a sensing device comprises at least one fluidic channel configured to receive a plurality of molecules to be detected, wherein at least some of the plurality of molecules are coupled to respective magnetic nanoparticles (MNPs), a plurality of magnetoresistive (MR) sensors, an insulating material encapsulating the plurality of MR sensors and for providing a barrier between the plurality of MR sensors and a contents of the at least one fluidic channel, and detection circuitry coupled to each of the plurality of MR sensors.
- MNPs magnetic nanoparticles
- MR magnetoresistive
- the detection circuitry comprises a bias element coupled to at least one of the plurality of MR sensors and configured to generate a bias across the at least one of the plurality of MR sensors, a first low pass filter and amplifier combination coupled to the at least one of the plurality of MR sensors to filter and amplify a signal from the at least one of the plurality of MR sensors, a reference oscillator configured to generate a reference signal having a particular frequency chosen to maximize a change in the signal at the particular frequency when at least one of the one or more MNPs labeling a particular molecule type is detected by the at least one of the plurality of MR sensors at one or more of the plurality of sites, a mixer coupled to the reference oscillator and an output of the first low pass filter and amplifier combination, wherein the mixer is configured to mix an output signal from the first low pass filter and amplifier combination with the reference signal, a second low pass filter
- the detection circuitry comprises a bias element coupled to at least one of the plurality of MR sensors and configured to generate a bias across the at least one of the plurality of MR sensors, an amplifier coupled to the at least one of the plurality of MR sensors to filter and amplify a signal from the at least one of the plurality of MR sensors, a filter coupled to the amplifier, and an envelope detector configured to receive an output signal from the filter and provide a signal for detection, wherein a voltage of the signal for detection is proportional to the fluctuation of the magnetic noise.
- the detection circuitry comprises a phase locked loop configured to provide an error signal output that corresponds to the phase of the magnetic noise.
- the sensing device further comprises a plurality of lines coupled to the plurality of MR sensors, and a plurality of selector elements, each of the plurality of selector elements coupled to at least one of the plurality of lines and to a respective one of the plurality of MR sensors.
- the plurality of selector elements comprises a transistor.
- the plurality of selector elements comprises an in-stack selector element.
- the sensing device is a sequencing device
- the molecules are biologic molecules (e.g., nucleic acid molecules).
- the sensing device further comprises a selector element, such as a transistor or an in-stack selector element.
- At least one of the MR sensors comprises a pinned layer, a free layer, and a spacer layer disposed between the pinned layer and the free layer, and an orientation of a magnetic moment of the free layer is approximately 90° from an orientation of a magnetic moment of the pinned layer
- a method of fabricating the sensing device comprises at least one of: applying a hard bias field; patterning the at least one of the MR sensors into a rectangle or ellipse; etching the free and pinned layers along an axis to induce texturing; or using perpendicular magnetic anisotropy to pull the free layer out of plane while keeping the pinned layer in the plane of the at least one of the MR sensors.
- a sensing device comprises at least one fluidic channel configured to receive a plurality of molecules to be detected, wherein at least some of the plurality of molecules to be detected are coupled to respective magnetic nanoparticles (MNPs), a plurality of magnetoresistive (MR) sensors, an insulating material encapsulating the plurality of MR sensors and for providing a barrier between the plurality of MR sensors and a contents of the at least one fluidic channel, and detection circuitry coupled to each of the plurality of MR sensors.
- MNPs magnetic nanoparticles
- MR magnetoresistive
- a surface of the insulating material within the fluidic channel provides a plurality of sites for binding the plurality of molecules to be detected, the plurality of sites being located among the plurality of MR sensors, and the detection circuitry is configured to detect a change in resistance, current, and/or voltage drop across each of the plurality of MR sensors, wherein the change in resistance, current, and/or voltage drop is influenced by the presence or absence of one or more MNPs at each of the plurality of sites.
- the detection circuitry is further configured to report the change in resistance, current, or voltage drop at each of the plurality of sites as a quantized output having one of a plurality of levels, at least some of the levels being used to differentiate MNPs having different saturation magnetizations, with each saturation magnetization corresponding to a particular MNP labeling a particular molecule type.
- the sensing device further comprises a plurality of lines coupled to the plurality of MR sensors, and a plurality of selector elements, each of the plurality of selector elements coupled to at least one of the plurality of lines and to a respective one of the plurality of MR sensors.
- the plurality of selector elements includes a transistor.
- the plurality of selector elements is an in-stack selector element.
- the sensing device is a sequencing device
- the molecules are biologic molecules (e.g., nucleic acid molecules).
- each of the MR sensors comprises a pinned layer, a free layer, and a spacer layer disposed between the pinned layer and the free layer, and, absent an applied magnetic field and absent the presence of one or more MNPs, an orientation of a magnetic moment of the free layer is approximately 90° from an orientation of a magnetic moment of the pinned layer.
- a first subset of the plurality of MR sensors is arranged in a first row
- a second subset of the plurality of MR sensors is arranged in a second row, the second row being substantially parallel to the first row
- the at least one fluidic channel is disposed between the first and second rows.
- the sensing device further comprises a selector element.
- the selector element comprises a transistor.
- the selector element is an in-stack selector element.
- the techniques described herein relate to a method of sensing molecules using a detection device, the detection device including a plurality of magnetoresistive (MR) sensors and at least one fluidic channel, the method including: adding a plurality of molecules to be detected to the at least one fluidic channel, wherein at least some of the plurality of molecules to be detected are coupled to respective magnetic nanoparticles (MNPs); detecting a characteristic of a magnetic noise of a first MR sensor of the plurality of MR sensors, wherein the characteristic of the magnetic noise is influenced by a presence of one or more MNPs in a vicinity of the first MR sensor; and determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor.
- MNPs magnetic nanoparticles
- the techniques described herein relate to a method, wherein the characteristic includes one or more of a level, a jitter, or a variance of the magnetic noise.
- the techniques described herein relate to a method, wherein causing the first MR sensor to produce a sensor signal includes: generating a bias across the first MR sensor.
- the techniques described herein relate to a method, wherein causing the first MR sensor to produce the sensor signal includes: applying a current to at least one line coupled to the first MR sensor.
- the techniques described herein relate to a method, wherein the characteristic of the magnetic noise is an amplitude of the magnetic noise at a particular frequency or within a particular frequency band, a fluctuation of the magnetic noise, or a phase of the magnetic noise.
- the techniques described herein relate to a method, wherein the characteristic of the magnetic noise is the amplitude of the magnetic noise at the particular frequency or within the particular frequency band, and wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: measuring the amplitude of the magnetic noise at the particular frequency or within the particular frequency band.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: lowpass filtering and amplifying the sensor signal; generating a reference signal having a selected frequency chosen to maximize a change in the sensor signal at the selected frequency in response to at least one of the one or more MNPs labeling a particular molecule type being detected by the first MR sensor; a mixer mixing the sensor signal and the reference signal; lowpass filtering and amplifying a mixer output signal from the mixer; providing the filtered and amplified mixer output signal to an envelope detector; and determining that the first MR sensor detected the presence of the one or more MNPs in the vicinity of the first MR sensor based on a change in an output of the envelope detector.
- the techniques described herein relate to a method, wherein the selected frequency is dependent on a type of the one or more MNPs.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: monitoring a detector output voltage; and determining, based on a change in the detector output voltage, that the first MR sensor detected the presence of the one or more MNPs in the vicinity of the first MR sensor.
- the techniques described herein relate to a method, wherein the characteristic is the fluctuation of the magnetic noise.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: monitoring a detector output voltage; and determining, based the detector output voltage being nonzero, that the first MR sensor detected the presence of the one or more MNPs in the vicinity of the first MR sensor.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: detecting changes over time in a detector output voltage.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: filtering the sensor signal; providing the filtered sensor signal to an envelope detector; and determining that the first MR sensor detected the presence of the one or more MNPs in the vicinity of the first MR sensor based on an output of the envelope detector being nonzero.
- the techniques described herein relate to a method, further including: amplifying the filtered sensor signal before providing the filtered sensor signal to the envelope detector.
- the techniques described herein relate to a method, wherein the characteristic is the phase of the magnetic noise.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs in the vicinity of the first MR sensor includes: providing an error signal output that corresponds to the phase of the magnetic noise.
- the techniques described herein relate to a method, further including: determining a baseline characteristic of the magnetic noise of the first MR sensor before adding the plurality of molecules to be detected to the at least one fluidic channel, and wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs within the fluidic channel includes: detecting a change in the magnetic noise of the first MR sensor relative to the baseline characteristic.
- the techniques described herein relate to a method, further including: applying a magnetic field across the sensing device; and detecting the characteristic of the magnetic noise of the first MR sensor.
- the techniques described herein relate to a method, wherein determining, based on the detected characteristic, whether the first MR sensor detected the presence of one or more MNPs within the fluidic channel includes: tracking an error signal of a phase locked loop (PLL).
- PLL phase locked loop
- FIG. 1 illustrates a portion of a magnetic sensor in accordance with some embodiments.
- FIGS. 2 A, 2 B, and 2 C illustrate the basic construction of a magnetoresistive (MR) device and how it can be used as a magnetic sensor in accordance with some embodiments.
- MR magnetoresistive
- FIGS. 3 A and 3 B illustrate the relationship between the resistance of the exemplary magnetic sensor illustrated in FIG. 1 and the angle between the moments of its two ferromagnetic layers in accordance with some embodiments.
- FIGS. 4 A, 4 B, and 4 C illustrate an apparatus for molecule detection in accordance with some embodiments.
- FIGS. 5 A, 5 B, 5 C, and 5 D illustrate portions of an exemplary apparatus that includes several channels in accordance with some embodiments.
- FIG. 5 E illustrates a magnetic sensor selection approach in accordance with some embodiments.
- FIG. 5 F illustrates another magnetic sensor selection approach in accordance with some embodiments.
- FIG. 6 is a flowchart illustrating a method of manufacturing an apparatus for molecule detection in accordance with some embodiments.
- FIG. 7 illustrates the results of each step of the method of manufacturing illustrated in FIG. 6 , with a final panel showing a polymerase bound to the edge of a magnetic sensor to be used to capture introduced nucleic acid bases such as DNA bases in accordance with some embodiments.
- FIGS. 8 A, 8 B, and 8 C illustrate a cross-point array architecture of MR sensor elements in accordance with some embodiments.
- FIGS. 9 A and 9 B illustrate a magnetic sensor and detection using that magnetic sensor in accordance with some embodiments.
- FIG. 10 A is a detection circuit in accordance with some embodiments.
- FIG. 10 B is another detection circuit in accordance with some embodiments.
- FIG. 11 is another detection circuit in accordance with some embodiments.
- the terms “over,” “under,” “between,” “on,” and other similar terms as used herein refer to a relative position of one layer with respect to other layers.
- one layer disposed over or under another layer may be directly in contact with the other layer or may have one or more intervening layers.
- one layer disposed between layers may be directly in contact with the two layers or may have one or more intervening layers.
- a first layer “on” a second layer is in contact with the second layer.
- the relative position of the terms does not define or limit the layers to a vector space orientation of the layers.
- Coupled is used herein to refer to elements that are either directly connected or connected through one or more intervening elements.
- a line e.g., for selecting or reading a characteristic of a magnetic sensor
- a line may be directly connected to a magnetic sensor, or it may be connected via intervening elements.
- the disclosures herein may be used to detect any type of molecule to which a magnetic particle can be attached.
- any molecule type that can be labeled by a magnetic nanoparticle may be detected using the sensing devices disclosed herein.
- Such molecule types may be biologic molecule types, such as proteins, antibodies, etc.
- the disclosures herein may be used to detect nucleic acids (e.g., in DNA sequencing).
- the disclosures herein may also be used to detect non-biologic (inorganic or non-living) molecules, such as contaminants, minerals, chemical compounds, etc.
- the presentation of the disclosure in the context of nucleic acid sequencing is solely exemplary and is not intended to limit the scope of the present disclosure.
- Suitable materials for use in the ferromagnetic layers 106 A, 106 B include, for example, alloys of Co, Ni, and Fe (sometimes mixed with other elements).
- alloys of Co, Ni, and Fe sometimes mixed with other elements.
- the example materials described above are merely exemplary and are not intended to be limiting. Materials suitable for use in MTJs are known to those having ordinary skill in the art.
- an incoming electric current spin polarized by the first FM layer (FM 1 ) 224 interacts differently with the second FM layer (FM 2 ) 228 , depending on the orientation of that layer's magnetic moment. If the moments of both FM layers 224 and 228 are parallel to one another ( FIG. 2 B ), then many electrons will pass through the device because many electrons in the current will have their spin oriented with the moment of the second FM 228 (spin 234 ). Few electrons will be reflected back (spin 232 ).
- the apparatus 100 is fabricated using photolithographic processes and thin film deposition.
- FIG. 6 illustrates a method 150 of manufacturing the apparatus 100
- FIG. 7 illustrates the results of each step of the fabrication method 150 with a final panel showing polymerase bound to the wall 117 proximate to a magnetic sensor 105 in accordance with some embodiments (e.g., when the apparatus 100 is used for nucleic acid sequencing).
- the method begins.
- the PLL 566 includes a signal generator 522 , which generates a clean RF signal based on a tuning input 524 .
- the tuning input 524 comes from components 526 and 528 forming a loop filter with an error amplifier 532 .
- the clean RF signal from the signal generator 522 is combined (mixed) with the signal coming from the amplifier 510 at a mixer 512 , and then filtered by a low pass filter 530 of the PLL 566 .
- the resultant error signal 534 of the PLL 566 is the magnetic noise of the magnetic sensor 105 , the characteristics of which depend on (e.g., are influenced or changed by) the presence or absence of a MNP.
- the error signal 534 can be used to detect the presence or absence of a MNP.
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Abstract
Description
| Magnetic | Expected | Expected | |||
| nanoparticle | minimum | maximum | Base | ||
| identity | resistance | resistance | labeled | ||
| MNP1 | R1 | <R2 | A | ||
| MNP2 | R2 | <R3 | T | ||
| MNP3 | R3 | <R4 | C | ||
| MNP4 | R4 | <R5 | G | ||
| Magnetic | Expected | Expected | |||
| nanoparticle | minimum | maximum | Base | ||
| identity | resistance | resistance | labeled | ||
| MNP1 | R1 | <R2 | A | ||
| MNP2 | R2 | <R3 | T | ||
| MNP3 | R3 | <R4 | C | ||
| MNP4 | Reference | Reference | G | ||
| (optionally | (optionally | ||||
| minus | plus | ||||
| tolerance) | tolerance) | ||||
Claims (20)
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| WO2020210370A1 (en) | 2019-04-12 | 2020-10-15 | Roche Sequencing Solutions, Inc. | Nucleic acid sequencing by synthesis using magnetic sensor arrays |
| US11747329B2 (en) | 2019-11-22 | 2023-09-05 | Western Digital Technologies, Inc. | Magnetic gradient concentrator/reluctance detector for molecule detection |
| US11791083B2 (en) * | 2021-05-26 | 2023-10-17 | Globalfoundries Singapore Pte. Ltd. | Tunnel magneto-resistive (TMR) sensor with perpendicular magnetic tunneling junction (p-MTJ) structures |
| US12211536B1 (en) * | 2022-07-31 | 2025-01-28 | Ceremorphic, Inc. | System and method for nanomagnet based logic device |
| JP7329783B1 (en) * | 2022-11-05 | 2023-08-21 | マグネデザイン株式会社 | magnetic microscope |
| US12499907B2 (en) * | 2023-05-05 | 2025-12-16 | Avago Technologies International Sales Pte. Limited | Systems for and methods for mode hop detection in heat assisted magnetic recording |
| JP7394425B1 (en) | 2023-08-11 | 2023-12-08 | マグネデザイン株式会社 | magnetic microscope |
| DE102023135655B4 (en) * | 2023-12-18 | 2025-07-10 | Infineon Technologies Ag | MAGNETORESISTIVE SENSOR |
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| US20210396820A1 (en) | 2021-12-23 |
| WO2020209911A1 (en) | 2020-10-15 |
| CN113227787B (en) | 2023-08-22 |
| US20200326391A1 (en) | 2020-10-15 |
| EP3953703A1 (en) | 2022-02-16 |
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| US11112468B2 (en) | 2021-09-07 |
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